Who is sponsoring CHUV-OVACURE?

CHUV-OVACURE is sponsored by Centre Hospitalier Universitaire Vaudois.

What condition does CHUV-OVACURE study?

CHUV-OVACURE studies Ovarian Carcinoma.

What drugs are being tested in CHUV-OVACURE?

Interventions: PEP-DC1, OC-DC, PEP-DC2, Low dose cyclophosphamide.

What is the status of CHUV-OVACURE?

CHUV-OVACURE is currently WITHDRAWN.

Last reviewed 2025-03-03 · How we verify

Phase I/II Study to Test the Immunogenicity, Feasibility, and Safety of Autologous PEP-DC Vaccine vs. Autologous OC-DC Vaccine Followed by PEP-DC Vaccine, in Combination With Low-dose Cyclophosphamide, in Patients With Advanced HGSOC (CHUV-OVACURE)

NCT05714306 Phase 1/Phase 2 WITHDRAWN

Single center, phase I/II randomized 2-arm study, evaluating two different vaccination regimens combined with low-dose cyclophosphamide in patients with advanced high grade serous ovarian carcinoma (HGSOC): * Arm A patients will be vaccinated with a personalized peptide vaccine comprised of autologous monocyte-derived dendritic cells (moDC) loaded with patient-specific peptides (PEP-DC1 vaccine) identified a priori at screening (8 patients); * Arm B patients will be vaccinated with a personalized tumor lysate vaccine comprising autologous moDC loaded with patient-specific autologous oxidized tumor lysate (OC-DC vaccine), followed by PEP-DC2 vaccine comprised of autologous moDC loaded with up to 10 patient-specific peptides identified midway through OC-DC vaccination (8 patients). In both arms, patients will receive a low dose cyclophosphamide the day before vaccination. Patients will be vaccinated after the end of adjuvant platinum-based chemotherapy, until vaccine exhaustion, disease recurrence, major toxicity or patient withdrawal, whichever is earlier.

Details

Lead sponsor	Centre Hospitalier Universitaire Vaudois
Phase	Phase 1/Phase 2
Status	WITHDRAWN
Start date	2023-08-01
Completion	2030-03

Conditions

Ovarian Carcinoma

Interventions

PEP-DC1
OC-DC
PEP-DC2
Low dose cyclophosphamide

Primary outcomes

Immunogenicity of OC-DC + PEP-DC vaccine vs. PEP-DC vaccine — through study completion, an average of 7 years
The number of personalized tumor antigen (PTAs) ranked as Top 100 will be identified for each patient before and after treatment and the difference will be compared between the two arms at least at two time-points, first at the end of the 3rd cycle (C3W3), and second, at end of treatment (EOT) visit (if possible at C6W4-W6 also). Specifically, an immunogenicity scoring will be determined as follows: for each of the 100 pre-determined top PTAs, a score will indicate how many peptides either become newly detected (shift from undetectable to detectable) or have a magnitude (frequency of T-cell directed against the epitope) increased by ≥ 2 fold.